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Pharmacokinetic-Pharmacodynamic modelling of intracellular Mycobacterium tuberculosis growth and kill rates is predictive of clinical treatment duration

机译:细胞内结核分枝杆菌生长和杀灭率的药代动力学-药效学模型可预测临床治疗时间

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摘要

Tuberculosis (TB) treatment is long and complex, typically involving a combination of drugs taken for 6 months. Improved drug regimens to shorten and simplify treatment are urgently required, however a major challenge to TB drug development is the lack of predictive pre-clinical tools. To address this deficiency, we have adopted a new high-content imaging-based approach capable of defining the killing kinetics of first line anti-TB drugs against intracellular Mycobacterium tuberculosis (Mtb) residing inside macrophages. Through use of this pharmacokinetic-pharmacodynamic (PK-PD) approach we demonstrate that the killing dynamics of the intracellular Mtb sub-population is critical to predicting clinical TB treatment duration. Integrated modelling of intracellular Mtb killing alongside conventional extracellular Mtb killing data, generates the biphasic responses typical of those described clinically. Our model supports the hypothesis that the use of higher doses of rifampicin (35 mg/kg) will significantly reduce treatment duration. Our described PK-PD approach offers a much needed decision making tool for the identification and prioritisation of new therapies which have the potential to reduce TB treatment duration.
机译:结核病(TB)的治疗时间长且复杂,通常需要联合服用6个月的药物。迫切需要改进药物方案以缩短和简化治疗,但是结核病药物开发的主要挑战是缺乏可预测的临床前工具。为了解决这一缺陷,我们采用了一种基于高含量成像的新方法,该方法能够确定一线抗结核药物对巨噬细胞内的细胞内结核分枝杆菌(Mtb)的杀伤动力学。通过使用这种药代动力学-药效学(PK-PD)方法,我们证明了细胞内Mtb亚群的杀灭动力学对于预测临床TB治疗持续时间至关重要。与常规细胞外Mtb杀灭数据一起的细胞内Mtb杀灭的集成模型可产生临床描述的典型两相反应。我们的模型支持以下假设:使用更高剂量的利福平(35 mg / kg)将显着缩短治疗时间。我们描述的PK-PD方法提供了急需的决策工具,用于确定新疗法并确定其优先级,从而有可能缩短结核病治疗时间。

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